Provided are gut microbes or cultures having anti-obesity efficacy and a pharmaceutical composition containing them. The gut microbes or cultures have anti-obesity efficacy by lowering fatty acid concentration of the gut fluid contents in a mammalian gastrointestinal tract for the prevention and treatment of obesity and obesity related diseases. This invention demonstrated that said gut microbes having anti-obesity efficacy by lowering fatty acid concentration of the gut fluid contents in the gastrointestinal tract of mammals have the anti-obesity efficacy as much as that of the representative anti-obesity drug, orlistat, without any side effects in animal experiments and clinical trials. Therefore, the gut microbes h can be used to develop universal anti-obesity drugs for obese patients, contributing greatly to the health of mankind.
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1. A method for promoting weight loss in a mammal by lowering fatty acid concentration of gut fluid in a gastrointestinal tract of the mammal, said method consisting of administering an effective amount of one or more strains selected from the group consisting of Lactobacillus reuteri JBD301 (KCTC 12606BP), Lactobacillus plantarum JBD302 (KCTC 12918BP), Lactobacillus casei JBD303 (KCTC 12919BP), Lactobacillus casei JBD304 (KCTC 12920BP), Lactobacillus paracasei JBD305 (KCTC 12921BP), Lactobacillus alimentarius JBD306 (KCTC 12922BP), Lactobacillus delbrueckii subsp. Lactis JBD307 (KCTC 12923BP), Lactobacillus pantheris JBD308 (KCTC 12924BP), Lactobacillus fermentum JBD309 (KCTC 12925BP), Lactobacillus rhamnosus JBD311 (KCTC 12926BP), Lactobacillus salivarius subsp. salicinius JBD312 (KCTC 12927BP), Lactobacillus mali JBD313 (KCTC 12928BP), Streptococcus lutetiensis JBD314 (KCTC 12929BP), and Lactococcus lactis subsp. Lactis JBD315 (KCTC 12930BP), or a culture thereof, to the mammal.
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This application is a National Stage of International Application No. PCT/KR2016/012791 filed Nov. 8, 2016, claiming priority based on Korean Patent Application No. 10-2015-0156733 filed Nov. 9, 2015, the contents of all of which are incorporated herein by reference in their entirety.
The present application relates to novel microorganisms having anti-obesity ability and pharmaceutical composition containing the same, particularly relates to novel gut microbes having anti-obesity efficacy by lowering fatty acid concentration and/or reducing fatty acid amounts of the gut fluid contents in a mammalian gastrointestinal tract for the prevention and treatment of obesity and obesity related diseases.
Obesity is an epidemic disease that is rarely curable and is increasing in prevalence in most of the world. It poses a major risk for various serious chronic diseases, such as metabolic syndrome, hypertension, type II diabetes, dyslipidemia, arteriosclerosis, ischemic heart disease, fatty liver disease, gallstones etc.
Because obesity is itself serious disease and causes cosmetic issues, intensive research has been conducted to develop anti-obesity pharmaceutical drugs. The main prescription products currently approved for obesity belongs to appetite suppressants or lipid digestion inhibitors.
Anti-obesity drugs through appetite suppression, such as fenfluramine, sibutramine, rimonabant, phentermine, acts on central nervous system, controlling appetite and therefore decreasing food intake. While appetite suppression drugs show great anti-obesity efficacy, many were withdrawn from the market due to severe side effects associated with sympathomimetic properties. Fenfluramine that led early anti-obesity market was discontinued in 1997 due to affection in heart rate and blood pressure. Also sibutramine (Meridia®, Reductil®) was discontinued in 2009 due to side effects such as increased heart rate. Rimonabant (Acomplia®, Sanofi-Aventis), launched in Europe, was discontinued in 2008 due to problems of serious mental illness such as depression and suicide. Recently, new anti-appetite drugs, phentermine/topiramate (Qsymia®) and lorcaserin (Belviq®), have been approved by FDA but its continuous marketing is not guaranteed since these anti-appetite drugs cannot avoid the occurrence of serious side effects after long-term use (Diabetes Metab J 2012; 36:13-25).
Orlistat (Xenical® and Alli® of Roche) is the only anti-obesity drug marketed successfully among lipid digestion inhibitor drugs for obesity. Orlistat is a gastric and pancreatic lipase inhibitor that prevents fat hydrolysis. Thus, administration of orlistat results in inhibition of fat digestion, reducing dietary fat absorption into the body but increasing fat excretion from the body. However, undigested fat along the gastrointestinal tract causes side effects such as diarrhea and fatty stool, which is not only uncomfortable but also socially unacceptable. Moreover, some report that long-term use of orlistat causes serious liver toxicity, causing US FDA review the safety of orlistat.
In conclusion, currently available anti-obesity drugs are not ideal and the social demand for obesity treatment that can treat obesity effectively without side effects is very high. Consequently, anti-obesity drugs with different modes of action without side effects are under active investigation all over the world. The most interesting approach among drug development through new paradigm is anti-obesity drugs using gut microbiota.
Obesity has been thought as a disease of energy balance, characterized by a chronic disequilibrium between energy intake and expenditure. Recent evidence showed that the gut microbiota plays an intricate role in the regulation of body weight and obesity (Nature 444:1027-31, Nature 474:327-36). The human digestive tract contains a complex diversity of bacteria, with over 1014 microbes which is more than 10 times of human cell numbers, interacting with human cells. Through interaction with human cells, gut microbes regulate absorption of food to human body and thus regulate the body weight and obesity of host. Theoretically, gut microbes have a tremendous advantage of excellent safety since they stay symbiotically in the intestine without being absorbed into the body. Thus, many efforts have been made to develop gut microbes as anti-obesity drugs with new mode of action (Current Pharmaceutical Design, 2009, 15:1546-1558).
U.S. Pat. No. 8,257,695 by Dupont provides satiety microbes, Lactobacillus acidophilus PTA 4797, Bacillus lactis 420, Bacillus lactis HN019 and Lactobacillus salivarius Ls-33 as anti-obesity agents.
U.S. Pat. No. 8,454,949 and 200601922 by Nestec provides t10c12-octadecadienoic acid producing Lactobacillus rhamnosus CNCM I-4046, U.S. Pat. Nos. 8,440,178 and 8,318,151 provides Lactobacillus rhamnosus NCC4007, U.S. Pat. No. 8,318,150 provides Lactobacillus helveticus CNCM I-4095, U.S. Pat. No. 8,637,000 provides Lactobacillus rhamnosus (ATCC53103), and EU Patent 2123168 provides Lactobacillus paracasei CNCM I-2116 as anti-obesity microbes.
U.S. Pat. No. 8,440,179 by Megamilk Snow Brand provides Lactobacillus gasseri SBT2055 and Lactobacillus helveticus SBT2171 as fat-reducing agents.
U.S. Pat. No. 7,001,756 by Genmont Niotech provides Lactobacillus rhamnosus GM-020 as anti-obesity agents. US patent 2009-0181437 by Yakult provides the conjugation method of linoleic acid to conjugated linoleic acid (CLA) and strains for that.
KR 2006-019222, EU Patent 1789531 and US Patent 2008-0267932 by CJ provides Lactobacillus rhamnosus PL60 (KCCM-10654P), converting linoleic acids to conjugated linoleic acid (CLA), as anti-obesity agents. US Patent 2008-0057044 by CJ provides Lactobacillus plantarum PL62 (KCCM-10655P), as anti-obesity agents.
KR Patent 543114 by Yakult provides Bacillus subtilis KY912 (KACC-91056) producing metabolites which inhibits α-glucosidase activity, as anti-obesity microbes. KR Patent 404236 by Bioneer provides Acetobacter sp. BC-Y058 and Lactobacillus sp. BC-Y009 which convert mono- and di-saccharides in the gut to polysaccharides for the prevention and treatment of diabetes and obesity. Bioneer also provides polysaccharide-producing Lactobacillus reuteri (KCTC-10301BP) in KR Patent 794701, Lactobacillus fermentum NM316 (KCTC-10458BP) in KR Patent 794702, and Lactobacillus gasseri BNR17 (KCTC 10902BP) in KR Patent 1108428.
Also, JINIS biopharmaceuticals, the assignee of this invention, provides fatty-acid absorbing Lactobacillus acidophilus FARM1 (KCTC 11513BP), FARM2 (KCTC 11514BP) and FARM3 (KCTC 11515BP) as anti-obesity agents in KR Patent 1292714.
However, all these anti-obesity microbes were effective in animal experiments but failed to successfully commercialized due to ineffective treatment and/or prevention in clinical trials.
Currently available anti-obesity drugs are chemical-based pharmaceuticals but not ideal with serious side effects. To solve this unmet need, research teams around the world are developing therapeutic agents for obesity using intestinal microorganisms. So far, however, all these anti-obesity microbes only demonstrate the possibility of treating obesity without side effects without success to develop pharmaceutical drugs using anti-obesity microbes.
Previous studies on the anti-obesity drug development using gut microbes have shown treatment in which gut microbes can control the satiety in the body, overproduce certain metabolites with anti-obesity effect, inhibit glycolysis, convert monosaccharides to polysaccharides, convert the general nutritional ingredients into anti-obesity substances (bioconversion) or promotes polysaccharide production. However, previous animal experiments and clinical trials only show that all these approaches were not effective to treat obesity.
Orlistat is the only anti-obesity drug approved for long-term use by healthcare departments of governments around the world. Orlistat, secreted into the gut content, is a pancreatic lipase inhibitor that prevents fat hydrolysis. Thus, administration of orlistat results in inhibition of fat digestion by inhibition of pancreatic lipase, reducing digestion of fat into absorbable fatty acids in the gut for obesity treatment. Based on this scientific observation, we have acknowledged that lowering the concentration of fatty acids in the gut fluid content using gut microbes can treat obesity as effective as orlistat. Unlike orlistat which cannot be free of side effect due to its property as chemicals, gut microbes have a tremendous advantage of inherent safety without side effect since they stay symbiotically in the intestine. Moreover, orlistat causes indigestion due to lipase inhibition activity while gut microbes specifically remove fatty acids in the gut without indigestion problem.
One object of this invention is to provide gut microbes having anti-obesity efficacy by lowering fatty acid concentration and/or reducing fatty acid amounts of the gut fluid contents in the gastrointestinal tract of mammals.
Another object of this invention is to provide functional foods and pharmaceuticals containing above microbes or cultures to prevent or treat obesity or obesity-related diseases.
To accomplish the said objects, the present invention provides novel gut microbes having anti-obesity efficacy by lowering fatty acid concentration and/or reducing the amount of fatty acids of the gut fluid contents in the gastrointestinal tract of mammals.
The present invention also provides pharmaceuticals containing above microbes or cultures having anti-obesity efficacy by lowering fatty acid concentration and/or reducing fatty acid amounts of the gut fluid contents in the gastrointestinal tract of mammals to prevent or treat obesity and obesity-related diseases.
The present invention also provides functional foods containing above microbes or cultures having anti-obesity efficacy by lowering fatty acid concentration and/or reducing fatty acid amounts of the gut fluid contents in the gastrointestinal tract of mammals to prevent or treat obesity and obesity-related diseases.
In this invention, said gut microbes can be selected from the groups that include, but are not limited to, Lactobacillus species, Streptococcus species, and Lactococcus species.
In this invention, said Lactobacillus species can be selected from the groups that include, but are not limited to, Lactobacillus reuteri, Lactobacillus plantarum, Lactobacillus casei, Lactobacillus paracasei, Lactobacillus alimentarius, Lactobacillus delbrueckii subsp. Lactis, Lactobacillus pantheris, Lactobacillus fermentum, Lactobacillus rhamnosus, Lactobacillus salivarius subsp. salicinius, Lactobacillus mali. and said Streptococcus species can be selected from the groups that include, but are not limited to, Streptococcus lutetiensis, and said Lactococcus species can be selected from the groups that include, but are not limited to, Lactococcus lactis subsp. Lactis.
In this invention, said Lactobacillus species can be selected from the groups that include, but are not limited to, Lactobacillus reuteri JBD301 (KCTC 12606BP), Lactobacillus plantarum JBD302 (KCTC 12918BP), Lactobacillus casei JBD303 (KCTC 12919BP), Lactobacillus casei JBD304 (KCTC 12920BP), Lactobacillus paracasei JBD305 (KCTC 12921BP), Lactobacillus alimentarius JBD306 (KCTC 12922BP), Lactobacillus delbrueckii subsp. Lactis JBD307 (KCTC 12923BP), Lactobacillus pantheris JBD308 (KCTC 12924BP), Lactobacillus fermentum JBD309 (KCTC 12925BP), Lactobacillus rhamnosus JBD311 (KCTC 12926BP), Lactobacillus salivarius subsp. salicinius JBD312 (KCTC 12927BP) and Lactobacillus mali JBD313 (KCTC 12928BP), said Streptococcus species can be selected from the groups that include, but are not limited to, Streptococcus lutetiensis JBD314 (KCTC 12929BP), and said Lactococcus species can be selected from the groups that include, but are not limited to, Lactococcus lactis subsp. Lactis JBD315 (KCTC 12930BP).
[Benefits]
This invention demonstrated that said gut microbes having anti-obesity efficacy by lowering fatty acid concentration and/or reducing the amount of fatty acids of the gut fluid contents in the gastrointestinal tract of mammals show the anti-obesity efficacy as much as that of the representative anti-obesity drug, orlistat, without any side effects in animal experiments and clinical trials.
Therefore, said gut microbes having anti-obesity efficacy by lowering fatty acid concentration and/or reducing the amount of fatty acids of the gut fluid contents in the gastrointestinal tract of mammals can be used to develop universal anti-obesity drugs for obese patients, contributing greatly to the health of mankind.
The currently available anti-obesity drugs have side effects or safety problems for long-term use. Previous attempts to develop safe anti-obesity drugs using appetite suppressant or lipase inhibitors have failed although the development is very urgent due to serious abuse problems with anti-obesity drugs.
Based on the understanding that previous anti-obesity drugs are absorbed into the body and causes various side effects due to the loss of appetite and inhibition of lipase inhibition, we attempted to confirm that symbiotic intestinal microorganisms that can reduce the fat absorption of the host can reduce obesity by reducing calorie intake.
Thus, in this invention, we conformed that 1) novel anti-obesity microbes were identified by screening intestinal microorganisms in the gastrointestinal tract, 2) novel anti-obesity microbes were colonized in the gastrointestinal tract of administered host, 3) novel anti-obesity microbes lowered the fatty acid concentration in the gut fluid content of host, 4) novel anti-obesity microbes reduced the absorption of dietary fat into the host but increase the secretion from the host, 5) novel anti-obesity microbes reduced the body weight of host.
Therefore, in the first aspect, the present invention relates to the gut microbes having anti-obesity efficacy by lowering fatty acid concentrations of the gut fluid contents in the gastrointestinal tract of mammals.
In this invention, said gut microbes can be selected from the groups that include, but are not limited to, Lactobacillus species, Streptococcus species, and Lactococcus species.
In this invention, said Lactobacillus species can be selected from the groups that include, but are not limited to, Lactobacillus reuteri, Lactobacillus plantarum, Lactobacillus casei, Lactobacillus paracasei, Lactobacillus alimentarius, Lactobacillus delbrueckii subsp. Lactis, Lactobacillus pantheris, Lactobacillus fermentum, Lactobacillus rhamnosus, Lactobacillus salivarius subsp. salicinius, Lactobacillus mali. and said Streptococcus species can be selected from the groups that include, but are not limited to, Streptococcus lutetiensis, and said Lactococcus species can be selected from the groups that include, but are not limited to, Lactococcus lactis subsp. Lactis.
In this invention, said Lactobacillus species can be selected from the groups that include, but are not limited to, Lactobacillus reuteri JBD301 (KCTC 12606BP), Lactobacillus plantarum JBD302 (KCTC 12918BP), Lactobacillus casei JBD303 (KCTC 12919BP), Lactobacillus casei JBD304 (KCTC 12920BP), Lactobacillus paracasei JBD305 (KCTC 12921BP), Lactobacillus alimentarius JBD306 (KCTC 12922BP), Lactobacillus delbrueckii subsp. Lactis JBD307 (KCTC 12923BP), Lactobacillus pantheris JBD308 (KCTC 12924BP), Lactobacillus fermentum JBD309 (KCTC 12925BP), Lactobacillus rhamnosus JBD311 (KCTC 12926BP), Lactobacillus salivarius subsp. salicinius JBD312 (KCTC 12927BP) and Lactobacillus mali JBD313 (KCTC 12928BP), said Streptococcus species can be selected from the groups that include, but are not limited to, Streptococcus lutetiensis JBD314 (KCTC 12929BP), and said Lactococcus species can be selected from the groups that include, but are not limited to, Lactococcus lactis subsp. Lactis JBD315 (KCTC 12930BP).
In a preferred embodiment of the invention, said gut microbes can be any microbes derived from human gut microbiota or gastrointestinal tract of mammals, can be in mammalian gastrointestinal tract, can lower the fatty acid concentrations in the gut fluid content of gastrointestinal tract, thereby reducing the absorption of dietary fat to the host.
Preferably, said gut microbes show the following 4 characteristics that can help to solve the side effect problems with the current anti-obesity drugs.
First, said gut microbes are not absorbed into the body but colonize in the gut and therefore there is no side effects caused by the absorption as in the case of chemical-based anti-obesity drugs. Second, said gut microbes are not acting on central nervous system and therefore there is no side effects caused by abuse or long-term use as in the case of appetite suppression drugs. Third, said gut microbes are not acting on fat digestion and therefore there is no side effects such as diarrhea, fatty stool, indigestion as in the case of lipase inhibition drugs. Forth, said gut microbes are safe and beneficial microorganisms and belongs to GRAS category.
In another aspect, the present invention relates to pharmaceutical compositions containing a gut microbe or culture with anti-obesity efficacy by lowering fatty acid concentrations in the gut fluid contents of in a mammalian gastrointestinal tract for the prevention or treatment of obesity or metabolic diseases caused by obesity.
In another aspect, the present invention relates to functional food composition containing a gut microbe or culture with anti-obesity efficacy by lowering fatty acid concentrations in the gut fluid contents of in a mammalian gastrointestinal tract for the prevention or treatment of obesity or metabolic diseases caused by obesity.
Preferably, said microbes or cultures contained in pharmaceutical or functional food compositions can lower fatty acid concentrations of the gut fluid contents more than 5%, and said gut may include stomach, small intestine and large intestine.
Preferably, said microbes or cultures may be contained, but not restricted, at dose of 103˜1012 cfu/gram in pharmaceutical or functional food compositions.
In this invention, said pharmaceutical compositions could be formulated, but not limited to, with more than 1 kind of pharmaceutically acceptable carrier in addition to said microbes or cultures having anti-obesity efficacy by lowering fatty acid concentrations of the gut fluid contents in the gastrointestinal tract.
In this invention, said functional foods are foods supplemented with functional ingredients and include, but not limited to, health food, nutraceuticals, dietary supplement, pharmabiotics. Preferably, said functional ingredients is for prevention and/or treatment of obesity and related metabolic syndrome.
Said functional foods include, but not limited to, dairy food (milk, soy milk, processed milk), fermented milk (drinking yogurt, set curd yogurt), drink, and soda. Said functional foods can include various supplementary components in addition to the functional ingredients. In the case of the functional food of the present invention, it is preferable to use additional supplements that include, but not limited to, vegetable creamer, skim milk powder, sugar, vitamin A, vitamin B1, vitamin B2, vitamin B3, vitamin B6, vitamin B12, folic acid, vitamin C, vitamin D3, Vitamins, and minerals such as copper, calcium, iron, magnesium, potassium, and zinc. In addition, said functional foods of the present invention may contain various flavors or natural carbohydrates as additional components as in the case of ordinary beverages. Said flavor agents may include natural sweeteners such as thaumatin and stevia extract, and synthetic sweeteners such as saccharin and aspartame. Said natural carbohydrates may include monosaccharides such as glucose and fructose, disaccharides such as maltose and sucrose, polysaccharides such as dextrin and cyclodextrin, and sugar alcohols such as xylitol, sorbitol and erythritol.
Said pharmaceuticals and functional foods in this invention contain said gut microbes having anti-obesity efficacy, and thus the administration of said pharmaceuticals and functional foods reduce the absorption of dietary fat into the host, contributing the prevention and/or treatment of obesity and related metabolic syndromes.
The technical idea of the present invention for the treatment of obesity can be applied to any gut microbes with anti-obesity efficacy by lowering fatty acid concentrations of the gut fluid contents in the gastrointestinal tract of mammals and will be apparent to those skilled in the art to which the present invention pertains.
The present invention may be better understood with reference to the accompanying examples that are intended for purposes of illustration only and should not be construed to limit the scope of the invention, as defined by the claims appended hereto.
By screening more than 20,000 strains with the said methods, we were able to find various gut microbes that can lower fatty acid concentration, followed by administration into mice for 12 weeks to measure the fatty acid concentration in the gut fluid contents and body weight changes of the host, as shown in
Experiment 1. Identification of Anti-Obesity Gut Microbes
The anti-obesity gut microbes, G5-1(JBD301), JBD302JBD309, JBD311-JBD315, were identified by screening as in Example 1. The taxonomic classification and phylogenetic analysis were based on the 16S rDNA gene and morphological observations. For morphological analysis, freshly cultured Lactobacillus was used for standard light microscopy after Gram staining as well as Transmission Electron Microscopy (TEM).
For 16S rRNA analysis, DNA was extracted from a G5-1 culture. For amplification of the 16s rDNA, PCR was performed in an automated thermal cycler with an initial denaturation at 95° C. for 5 min, followed by 30 cycles at 95° C. for 30 sec, 52° C. for 45 sec, 72° C. for 2 min, and then 72° C. for 10 min. For amplification of the 16s rDNA, universal primers (SEQ ID NO: 1 and SEQ ID NO: 2) were selected
[SEQ ID NO: 1] 27 F: 5′-AGA GTT TGA TCC TGG CTC AG-3′
[SEQ ID NO: 2] 1492R: 5′-GGT TAC CTT GTT ACG ACT T-3′
The obtained 16s rDNA sequences (SEQ ID NOS: 3-16) of G5-1(JBD301), JBD302-JBD309, and JBD311-JBD315 were used to identify homologous sequences by searching the NCBI GenBank, DNA data bank of Japan, European Nucleotide Archive. After confirming novel species of the above microbes, G5-1(JBD301) were deposited as NCBI GenBank Accession number KJ957189.
Experiment 2. Acid Production of Anti-Obesity Gut Microbes
To test acid production, JBD301 microbe was cultured at 37° C. in MRS broth. The cell culture was inoculated into bottles containing 100 ml of sterile reconstituted skim milk (10%) and glucose (2%). The pH changes of the fermented milk were determined after incubation for 24, 48 and 72 h. The average value with 10 samples per group was indicated as mean±standard deviation, as shown in Table 1.
TABLE 1
Time (hr)
JBD 301-fermented yogurt pH
24
4.404 ± 0.034
48
4.092 ± 0.059
72
4.048 ± 0.012
As shown in Table 1, pH reduction by acid production was observed.
Experiment 3. In Vitro Evaluation of Lowering Fatty Acid Concentration by Anti-Obesity Gut Microbes
JBD301 was inoculated onto MRS agar for incubation at 37° C. in anaerobic jar (Gas-Pack anaerobic systems, BBL). After 48 hours, colonies on MRS agar were inoculated into MRS media in 96-well plate for anaerobic incubation at 37° C. The obtained culture was subjected to EnzyChrom™ FFA Assay Kit (Bio-Assay Systems) as in Example 1. The amount of fatty acid in the supernatant was determined with EnzyChrom™ FFA Assay Kit (Bio-Assay Systems) using absorbance at 570 nm and the capacity of lowering fatty acid concentration by JBD301 was shown in
As shown in
Experiment 4. In Vivo Evaluation of Lowering Fatty Acid Concentration in the Gut Fluid Content by Anti-Obesity Gut Microbes
Lactobacillus colonize in the small intestine, where fatty acids, digestion products of lipid, are mainly absorbed in the body. The decrease in the amount of fatty acids in the small intestine where most of the fatty acid is absorbed reduces the amount of fat that can be absorbed by the human body, thus reducing the caloric intake of the host. To confirm this, the concentration and amount of fatty acids in the intestinal fluid (gut fluid content) were measured.
Six-week-old C57BL/6 female mice (Joongang Experimental Animal Co., Seoul, Korea) were housed at 7 animals per cage with food (10% fat; D12450B; Research Diets Inc., New Brunswick, N.J., USA) and water available ad libitum under a 12-h light/12-h dark cycle at 22° C. and 55% humidity. After 1 week of acclimation, mice were randomly divided into with control or experimental group. Control mice were fed high-fat diet (45% kcal as fat, D12451, Research Diets Inc.) while experimental mice fed high-fat diet supplemented daily with 107 CFU of JBD301 for 3 weeks. After 3-week administration of Lactobacillus, mice were sacrificed under anesthesia. Both total fluid contents from small and large intestine were collected immediately and weighed. The gut fluid contents were collected with known volume of sterile saline. Then, the samples in saline were centrifuged at 10,000×g for 30 min. After centrifugation, the supernatant was collected and analyzed for total FFAs content using the EnzyChrom™ Free Fatty Acid Assay Kit (Bio-Assay Systems), as shown in
Experiment 5. In Vivo Evaluation of Lowering Fatty Acid Absorption and Increasing Fatty Acid Excretion by Anti-Obesity Gut Microbes
To evaluate lowering of fatty acid absorption in the host after administration of JBD301, mice were fed high-fat diet supplemented with JBD301 for 3 weeks and then 14C-radiolabeled triolein was orally administered as in Experiment 4. Blood was collected at times (2 h˜96 h), mixed with liquid scintillation cocktail, and radioactivity from 14C was measured with Microplate Scintillation Counter (PerkinElmer), as shown in
Also, feces were collected to evaluate the excretion amount of fatty acid from the host after administration of JBD301. Fecal samples at times were added to Solvable™ (PerkinElmer), mixed for 1 hour at 60° C., and bead homogenized samples were centrifuged at 13,000 rpm for 5 minutes. Then, the supernatant was added with 1/10 (v/v) H2O2, mixed for 10 minutes at 50° C. and centrifuged at 13,000 rpm for 5 minutes. The obtained supernatant was added with liquid scintillation cocktail and 14C radioactivity was measured with Microplate Scintillation Counter (PerkinElmer).
All animal care and use were performed strictly in accordance with the ethical guidelines by the Institutional Animal Care and Use Committee. Six-week-old C57BL/6 female mice (Joongang Experimental Animal Co., Seoul, Korea) were housed at 10 animals per cage with food (10% fat; D12450B; Research Diets Inc., New Brunswick, N.J., USA) and water available ad libitum under a 12-h light/12-h dark cycle at 22° C. and 55% humidity. After 1 week of acclimation, mice were randomly divided into with control or experimental groups. Control mice were fed high-fat diet (45% kcal as fat, D12451, Research Diets Inc.), JBD301 group fed high-fat diet supplemented with 107 CFU of JBD301, and orlistat group fed high-fat diet supplemented with orlistat (Xenical®, Roche) 50 mg/kg diet. Body weight changes were monitored for 4-week administration as shown in
As shown in
Phase 2 clinical trials were performed to validate the efficacy of JBD301 as anti-obesity microbes (Clinical Research Information Service of Korea as KCT0000452). This is to determine whether the intake of JBD301 in overweight or obese subjects is effective in reducing body weight or body fat. The clinical trial design of JBD301 is shown in
Participating subjects were recruited according to clinical trial protocols approved by the IRB. Study participants were enrolled for the study if they satisfied the following criteria: 1) written informed consent, 2) men or women 25-65 years of age, and 3) body mass index of 25-35 kg/m2. The exclusion criteria included the following: subjects who received antibiotics within 12 weeks prior to the first visit; subjects with current use of medications for body weight reduction (lipase inhibitors, anti-depressants, appetite suppressants), diuretics, contraceptives, steroids, and hormones; subjects who were involved in commercial diet programs or were under a diet formula within 12 weeks prior to the first visit; subjects with uncontrolled hypertension or diabetes; subjects with current medical conditions including cardiac, renal, hepatic, neurovascular, thyroid or parathyroid disorders/diseases; subjects with medical conditions including depression, schizophrenia, psychosis, alcohol abuse or drug abuse; subjects diagnosed with cancer within the past 5 years; subjects with hyper-allergic reactions to components in the testing food; subjects who were planning to reduce body weight by food and exercise during the clinical trial period; and subjects that were pregnant or breast-feeding.
The subjects were instructed to maintain their usual diet with no intake of probiotics, antibiotics or agents known to affect body weight. The enrolled subjects were simply randomized for parallel assignment. The study consisted of daily administration of 1 capsule of either Lactobacillus JBD301 (10[9] CFU) or placebo for 12 weeks without any dietary restriction. In a capsule of 450 mg, major ingredient, either JBD301 powder or non-dairy coffee creamer, is 12% while other excipients include 40% skim milk, 40% sucrose and 8% ascorbic acid.
TABLE 2
Group
Variable
L. reuteri JBD301
Control
P value
All participants
18 (48.6)
19 (51.4)
0.103
Sex, male
7 (38.9)
13 (68.4)
Sex, female
11 (61.1)
6 (31.6)
Age mean ± SEM
39.4 ± 2.7
42.1 ± 3.1
0.578
Height mean ± SEM
165.0 ± 2.4
169.0 ± 2.3
0.233
Weight mean ± SEM
79.6 ± 3.4
80.1 ± 3.0
0.822
BMI mean ± SEM
29.0 ± 0.7
27.9 ± 0.5
0.150
The primary outcome from this study was body weight in obese adults. The adipose tissue area and body fat mass of each subject were measured using computerized tomography (CT) and Dual-Emission X-ray Absorptiometry (DEXA), respectively. For the clinical data, the statistical analysis was performed using procedures in SAS (Version 9.2) and MedCalc (Version 11.6.0). Depending on the normality of the underlying data, the Mann-Whitney U test and the Wilcoxon Signed Rank test were used to perform statistical analyses.
The Mann-Whitney U test was used to compare the outcome variables. The percentage change in outcome variables at 12 weeks (%) was calculated by the following formula: ((value at 12 weeks—value at 0 week)/value at 0 week)×100. Without any dietary restrictions or additional exercise, changes in the body weight from baseline to endpoint were 0.31% (0.21 kg) in the Lactobacillus JBD301 group and 1.77% (1.45 kg) in the placebo group, resulting in a 1.46% (1.24 kg) between-group difference. A Mann-Whitney U test showed that there was a statistically significant difference in the percentage change of weight between the Lactobacillus JBD301 and the placebo group (P=0.026) as well as in the BMI (P=0.036) from the 0 week assessment to the 12 weeks assessment.
TABLE 3
(Unit: %)
L. reuteri JBD301
Control
Mean ±
Mean ±
% change in Variable
n
SEM
n
SEM
P value
Total abdominal Fat
18
1.64 ± 4.26
19
3.45 ± 4.23
1.000
area (cm2)
Body fat mass (g)
18
−0.38 ± 2.09
19
3.41 ± 1.17
0.053
Weight (kg)
18
0.31 ± 0.71
19
1.77 ± 0.40
0.026*
BMI (kg/m2)
18
0.32 ± 0.76
19
1.65 ± 0.46
0.036*
Hip circumstance (cm)
18
−0.20 ± 0.45
19
0.76 ± 0.31
0.126
HbA1c (%)
18
−1.61 ± 1.02
19
1.39 ± 1.16
0.118
*P values were obtained from Mann-Whitney U test, significant difference if P value is ≤ 0.05.
The Wilcoxon Signed Rank test was used to compare the percentage differences in outcome variables for the two treatment groups. The percentage differences in outcome variables were calculated by the following formula: (value of experimental/value of placebo)×100. Wilcoxon Signed Rank test confirmed that there was a statistically significant difference in the pairwise comparison of the percentage between 97.94% of JBD301 group (n=18) and 100% of control group (n=19)(P=0.028).
TABLE 4
(Unit: %)
0 week
12 week
P value
% control in body weight
99.45 ± 4.26
97.94 ± 4.21
0.028*
*P values were obtained from Wilcoxon signed rank test, significant difference if P value is ≤ 0.05. Values are mean ± SEM.
According to the present invention, the use of an intestinal strain having the ability to inhibit obesity by reducing the concentration of fatty acid dissolved in gut fluid content in the mammalian gastrointestinal tract enables the development of an anti-obesity drug that can be generally utilized by patients already suffering from obesity, whereby a significant contribution to human health can be expected.
Kim, Hyeon Jin, Hong, Seong Tshool, Yu, Jae Gak
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